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聚集蛋白抑制神经突生长,但促进胚胎运动神经元和感觉神经元的附着。

Agrin inhibits neurite outgrowth but promotes attachment of embryonic motor and sensory neurons.

作者信息

Chang D, Woo J S, Campanelli J, Scheller R H, Ignatius M J

机构信息

Department of Molecular and Cell Biology, University of California, Berkeley 94720-3200, USA.

出版信息

Dev Biol. 1997 Jan 1;181(1):21-35. doi: 10.1006/dbio.1996.8435.

Abstract

Agrin is a secreted glycoprotein with the ability to cluster cell surface molecules, including the nicotinic acetylcholine receptor (AchR) on muscle cells. Alternate splicing of agrin mRNA results in a family of agrin proteins which differ in their clustering potency. Neuronal-specific isoforms with the highest clustering activity play a role in clustering postsynaptic proteins at the neuromuscular junction. However, the function of agrin isoforms expressed in many nonneuronal tissues, and only weakly active in clustering assays, remains obscure. Monolayer cultures of Chinese hamster ovary (CHO) cells expressing a neuronal (agrin-19) or a nonneuronal (agrin-0) form of agrin were used to assay the effect of agrin on neurite outgrowth and cell attachment. These results were compared to outgrowth on control CHO cells expressing only drug resistance and on regions of CHO-agrin monolayers not expressing detectable levels of agrin. Neurite extension on confluent monolayers of agrin-0- or -19-expressing CHO cells was reduced substantially below that of controls. In one experiment neurite lengths were compared at 2 and 3 days after plating and suggested that neurite outgrowth may be stopped and not simply retarded. Attachment of sensory or motoneurons was nearly twofold higher to agrin monolayers than to control cells, showing that the inhibition is not a result of a nonpermissive environment. An agrin construct missing the C-terminal half, removing the major site of variability and clustering activity, was also tested. This construct did not reduce outgrowth, suggesting that the C-terminal half of the protein may be important in stopping growth as well as inducing clustering. These results expand the role of agrin in synaptogenesis as it may provide a stop signal at the myofiber surface and may anchor the presynaptic fibers to the eventual motor endplate .

摘要

集聚蛋白是一种分泌型糖蛋白,能够使细胞表面分子聚集,包括肌肉细胞上的烟碱型乙酰胆碱受体(AchR)。集聚蛋白mRNA的可变剪接产生了一系列集聚蛋白,它们的聚集能力各不相同。具有最高聚集活性的神经元特异性异构体在神经肌肉接头处的突触后蛋白聚集中发挥作用。然而,在许多非神经元组织中表达且在聚集试验中活性较弱的集聚蛋白异构体的功能仍不清楚。利用表达神经元形式(集聚蛋白-19)或非神经元形式(集聚蛋白-0)的中国仓鼠卵巢(CHO)细胞单层培养物来检测集聚蛋白对神经突生长和细胞附着的影响。将这些结果与仅表达耐药性的对照CHO细胞以及不表达可检测水平集聚蛋白的CHO-集聚蛋白单层区域上的生长情况进行比较。在表达集聚蛋白-0或-19的CHO细胞汇合单层上,神经突延伸明显低于对照组。在一项实验中,比较了接种后2天和3天的神经突长度,结果表明神经突生长可能停止而不仅仅是受到抑制。感觉神经元或运动神经元与集聚蛋白单层的附着比与对照细胞的附着高出近两倍,这表明这种抑制不是由于非允许环境导致的。还测试了一个缺失C端一半、去除了主要可变位点和聚集活性位点的集聚蛋白构建体。该构建体并未减少生长,这表明该蛋白的C端一半可能在停止生长以及诱导聚集方面都很重要。这些结果扩展了集聚蛋白在突触形成中的作用,因为它可能在肌纤维表面提供一个停止信号,并可能将突触前纤维锚定到最终的运动终板上。

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